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A new age for biomedical applications of Ribosome Inactivating Proteins (RIPs): from bioconjugate to nanoconstructs

机译:核糖体失活蛋白(RIPs)在生物医学应用中的新纪元:从生物结合物到纳米结构

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摘要

Ribosome-inactivating proteins (RIPs) are enzymes (3.2.2.22) that possess N-glycosilase activity that irreversibly inhibits protein synthesis. RIPs have been found in plants, fungi, algae, and bacteria; their biological role is still under investigation, even if it has been recognized their role in plant defence against predators and viruses. Nevertheless, several studies on these toxins have been performed to evaluate their applicability in the biomedical field making RIPs selectively toxic towards target cells. Indeed, these molecules are extensively used to produce chimeric biomolecules, such as immunotoxins or protein/peptides conjugates. However, to date, clinical use of most of these bioconiujates has been limited by toxicity and immunogenicity. More recently, material sciences have provided a wide range of nanomaterials to be used as excellent vehicles for toxin-delivery, since they are characterized by improved stability, solubility, and in vivo pharmacokinetics. This review discusses progresses in the development of RIPs bioconjugates, with particular attention to the recent use of nanomaterials, whose appropriate design opens up a broad range of different possibilities to the use of RIPs in novel therapeutic approaches in human diseases.
机译:核糖体失活蛋白(RIP)是具有N-糖基甲硅烷酶活性的酶(3.2.2.22),该酶不可逆地抑制蛋白质合成。在植物,真菌,藻类和细菌中发现了RIP。即使已经认识到它们在植物防御天敌和病毒中的作用,它们的生物学作用仍在研究中。然而,已经进行了关于这些毒素的数项研究以评估它们在生物医学领域中的适用性,从而使RIP对目标细胞具有选择性毒性。实际上,这些分子被广泛用于产生嵌合生物分子,例如免疫毒素或蛋白质/肽结合物。然而,迄今为止,大多数这些生物连接物的临床使用受到毒性和免疫原性的限制。最近,材料科学提供了广泛的纳米材料,可被用作出色的毒素传递载体,因为它们的特点是稳定性,溶解性和体内药代动力学提高。这篇综述讨论了RIPs生物共轭物的开发进展,特别关注了纳米材料的最新使用,纳米材料的适当设计为人类疾病在新型治疗方法中使用RIPs开辟了广泛的不同可能性。

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